Bellas Olivia M, Cao Katrina, Bowen Joanne, Smid Scott, Shakib Sepehr, Crawford Gregory B, Zannettino Andrew, Yeung David T, Kichenadasse Ganessan, Boublik Jarosalv, Louise Jennie, Marker Julie, Cambareri Bronwyn, Price Timothy, Wardill Hannah R
School of Biomedicine, University of Adelaide, Adelaide, South Australia, Australia.
Supportive Oncology Research Group, Precision Cancer Medicine Theme, South Australian Health and Medical Research Institute, Adelaide, South Australia, Australia.
BMJ Open. 2025 Mar 3;15(3):e089336. doi: 10.1136/bmjopen-2024-089336.
Many chemotherapy agents used to treat advanced cancer are inherently mucotoxic, causing breakdown of the gastrointestinal mucosa (gastrointestinal mucositis (GI-M)) and lead to a constellation of secondary complications including diarrhoea, malnutrition, anorexia, pain, fatigue and sleep disturbances. These symptoms are usually managed individually, leading to polypharmacy and its associated risks. The endocannabinoid system regulates numerous biological and behavioural processes associated with chemotherapy side effects, suggesting its modulation could control these symptoms. Therefore, the CANnabinoids in CANcer (CANCAN) therapy trial is a phase II, randomised, double-blind, placebo-controlled trial that aims to determine the efficacy of medicinal cannabis in minimising GI-M and its associated symptom burden.
The CANCAN trial is being conducted at four Australian sites: the Royal Adelaide Hospital, the Queen Elizabeth Hospital, Flinders Medical Centre and the Lyell McEwin Hospital. Adults (n=176) diagnosed with a solid tumour or a haematological cancer scheduled to receive mucotoxic chemotherapy will be eligible. Participants will be randomised 1:1 to receive either the investigational product (IP) or placebo, both delivered as sublingual wafers. The active IP contains cannabidiol (300 mg/day) and Δ-tetrahydrocannabinol (5-20 mg/day, titrated by the participant). The primary outcome is GI-M burden, determined by the Mucositis Daily Questionnaire. Secondary and tertiary outcomes include overall symptom burden (Edmonton Symptom Assessment Scale), anorexia (Average Functional Assessment of Anorexia/Cachexia Therapy), depression/anxiety (Hospital Anxiety and Depression Scale), financial toxicity (Functional Assessment of Chronic Illness Therapy COmprehensive Score for financial Toxicity), quality of life (European Organisation for Research and Treatment of Cancer Core Quality of Life Questionnaire), incidence of chemotherapy dose reductions/modifications, cumulative dose of chemotherapy administered, incidence/length of hospitalisation, the use of supportive care, and the cost-benefit of the IP. The CANCAN trial prioritises patient experiences by focusing on patient-reported outcome measures and administering medicinal cannabis during active treatment to prevent symptoms that occur secondary to mucositis.
The protocol has been approved by Central Adelaide Local Health Network Human Research Ethics Committee (2022HRE00037). All participants will be required to provide written or digitally authorised informed consent. Trial results will be disseminated in peer-reviewed journals, and at scientific conferences.
ACTRN12622000419763.
许多用于治疗晚期癌症的化疗药物本质上具有黏膜毒性,会导致胃肠道黏膜破损(即胃肠道黏膜炎(GI-M)),并引发一系列继发性并发症,包括腹泻、营养不良、厌食、疼痛、疲劳和睡眠障碍。这些症状通常是分别进行处理,导致了多药联用及其相关风险。内源性大麻素系统调节着许多与化疗副作用相关的生物学和行为过程,这表明对其进行调节可能会控制这些症状。因此,癌症中的大麻素(CANCAN)治疗试验是一项II期随机双盲安慰剂对照试验,旨在确定药用大麻在减轻胃肠道黏膜炎及其相关症状负担方面的疗效。
CANCAN试验在澳大利亚的四个地点进行:阿德莱德皇家医院、伊丽莎白女王医院、弗林德斯医疗中心和莱尔·麦克尤恩医院。确诊患有实体瘤或血液系统癌症且计划接受黏膜毒性化疗的成年人(n = 176)符合条件。参与者将按1:1随机分组,分别接受研究产品(IP)或安慰剂,两者均以舌下含片的形式给药。活性IP包含大麻二酚(300毫克/天)和Δ-四氢大麻酚(5 - 20毫克/天,由参与者滴定)。主要结局是胃肠道黏膜炎负担,通过黏膜炎每日问卷确定。次要和三级结局包括总体症状负担(埃德蒙顿症状评估量表)、厌食(厌食/恶病质治疗的平均功能评估)、抑郁/焦虑(医院焦虑抑郁量表)、经济毒性(慢性病治疗功能评估财务毒性综合评分)、生活质量(欧洲癌症研究与治疗组织核心生活质量问卷)、化疗剂量减少/调整的发生率、给予的化疗累积剂量、住院发生率/时长、支持性护理的使用情况以及IP的成本效益。CANCAN试验通过关注患者报告的结局指标并在积极治疗期间给予药用大麻以预防黏膜炎继发的症状,将患者体验放在首位。
该方案已获得阿德莱德中央地方卫生网络人类研究伦理委员会批准(2022HRE00037)。所有参与者都需要提供书面或数字授权的知情同意书。试验结果将在同行评审期刊和科学会议上公布。
ACTRN12622000419763。
